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1 phorylation decreased in the presence of (+)-pentazocine.
2 fect was decreased by the application of (+)-pentazocine.
3 n the Ins2Akita/+ mice were treated with (+)-pentazocine.
4 stress, but decreased in the presence of (+)-pentazocine.
5 typic sigma-1 agonists (+)-SKF10,047 and (+)-pentazocine.
6 ocine > DTG (1, 3-di-o-tolylguanidine) > (-)-pentazocine.
7 e animals were randomized to four groups: a) pentazocine (0.3 mg/kg), a delta-opioid receptor agonist
15 ophysis the sigma receptor ligands SKF10047, pentazocine, and ditolylguanidine all reversibly inhibit
16 m Ins2Akita/+ diabetic mice treated with (+)-pentazocine, and the expression of ER stress genes and o
17 the prototypical sigma receptor agonist (+)-pentazocine, and the proposed endogenous sigma receptor
19 p of chemically unrelated ligands, including pentazocine, apomorphine (a dopamine receptor agonist) a
23 ed by dehydroepiandrosterone sulfate and (+)-pentazocine but not by (-)-pentazocine, the synthetic (-
26 sigma-1 receptor was identified by (+)-[(3)H]pentazocine competitive binding with nonradioactive [(12
27 The primary effect of dextromethorphan, (+)-pentazocine, (+)-cyclazocine, (+)-SKF10047, carbetapenta
28 eptor (Sigma1R), and the Sigma1R agonist (+)-pentazocine did not compete for high-affinity binding.
29 tent with its low potency at p38 activation, pentazocine did not produce conditioned place aversion i
30 two known Sig1R ligands, haloperidol and (+)-pentazocine, disrupted the Nav1.5/Sig1R interaction both
31 te drugs (fentanyl, morphine, buprenorphine, pentazocine) followed by 2 hours of 34 degrees C ischemi
32 e received intraperitoneal injections of (+)-pentazocine for 22 weeks beginning at diabetes onset.
33 reserved in the morphine, buprenorphine, and pentazocine groups when compared with cardioplegia alone
34 nyl)ethylamine) > 4-IPBS > haloperidol > (+)-pentazocine > DTG (1, 3-di-o-tolylguanidine) > (-)-penta
36 ts in which (-)-PTZ, the levo-isomer form of pentazocine, had no neuroprotective effect on excitotoxi
37 etic small molecules, including cocaine, (+)-pentazocine, haloperidol, and small endogenous molecules
39 hexane-1-carboxylate hydrochloride), and (+)-pentazocine increases the expression of GluN2A and GluN2
40 h selective sigma(1)R agonists (PRE-084, (+)-pentazocine) lacked reinforcing effects in drug-naive ra
41 systems because the final sigma agonist (+)-pentazocine lowered opioid analgesia in all mice, includ
42 R1 binds BiP under stressful conditions; (+)-pentazocine may exert its effects by dissociating sigmaR
43 ls, and the effect of the sigmaR1 ligand (+)-pentazocine on pro- and anti-apoptotic and endoplasmic r
47 uP734, haloperidol and DTG) that reverse (+)-pentazocine- or BD737-mediated inhibition, as well as a
48 morphone, methadone, oxycodone, papaveretum, pentazocine, pethidine, tapentadol, and tramadol) to tre
49 rt that the prototypical sigma1R agonist (+)-pentazocine potentiated the dose response of cocaine sel
50 F4, and NE100) and 4 sigma(1) agonists ((+)-pentazocine, (+/-)-PPCC, PRE-084, and (+)-SKF10047) were
51 mg/kg), a delta-opioid receptor agonist; b) pentazocine pretreated with KATP channel blocker, gliben
53 and demonstrated that the sigmaR1 ligand (+)-pentazocine ((+)-PTZ) could protect against cell death.
54 ration of the high-affinity Sig1R ligand (+)-pentazocine [(+)-PTZ] to rd10 mice over several weeks le
56 s using the sigma-1-selective ligand [3H](+)-pentazocine showed a high-affinity binding (Kd = 5.80 nM
57 e sulfate and (+)-pentazocine but not by (-)-pentazocine, the synthetic (-)-enantiomer of PREGS or th
60 architecture; IPL and INL thicknesses of (+)-pentazocine-treated Ins2(Akita/+) mouse retinas were wit
67 of defibrillation, the beneficial effects of pentazocine were abolished by pretreatment with the KATP
68 ligands, 1,3-di(2-tolyl)guanidine (DTG) and pentazocine, were shown to induce c-fos in similar patte
69 reported that the opioid agonist-antagonist pentazocine, which acts predominantly at kappa-receptors